DMBT1 Encodes a Protein Involved in the Immune Defense and in Epithelial Differentiation and is Highly Unstable in Cancer

Overview

Journal Cancer Res

Specialty Oncology

Date 2000 Apr 5

PMID 10749143

Citations 63

Authors

J Mollenhauer

S Herbertz

U Holmskov

M Tolnay

I Krebs

A Merlo

H D Schroder

D Maier

F Breitling

S Wiemann

H J Grone

A Poustka

Affiliations

Soon will be listed here.

Abstract

The gene deleted in malignant brain tumors 1 (DMBT1) has been proposed as a candidate tumor suppressor for brain, gastrointestinal, and lung cancer. It codes for a protein of unknown function belonging to the superfamily of scavenger receptor cysteine-rich proteins. We aimed at getting insights into the functions of DMBT1 by expression analyses and studies with a monoclonal antibody against the protein. The DMBT1 mRNA is expressed throughout the immune system, and Western blot studies demonstrated that isoforms of DMBT1 are identical to the collectin-binding protein gp-340, a glycoprotein that is involved in the respiratory immune defense. Immunohistochemical analyses revealed that DMBT1 is produced by both tumor-associated macrophages and tumor cells and that it is deregulated in glioblastoma multiforme in comparison to normal brain tissue. Our data further suggest that the proteins CRP-ductin and hensin, both of which have been implicated in epithelial differentiation, are the DMBT1 orthologs in mice and rabbits, respectively. These findings and the spatial and temporal distribution of DMBT1 in fetal and adult epithelia suggest that DMBT1 further plays a role in epithelial development. Rearrangements of DMBT1 were found in 16 of 18 tumor cell lines, and hemizygous deletions were observed in a subset of normal individuals, indicating that the alterations in tumors may be a result of both pre-existing deletions uncovered by a loss of heterozygosity and secondary changes acquired during tumorigenesis. Thus, DMBT1 is a gene that is highly unstable in cancer and encodes for a protein with at least two different functions, one in the immune defense and a second one in epithelial differentiation.

Citing Articles

Search for germline gene variants in colorectal cancer families presenting with multiple primary colorectal cancers.

Forsti A, Ambrozkiewicz F, Marciniak M, Lubinski J, Hemminki K Int J Cancer. 2024; 156(7):1393-1403.

PMID: 39654522 PMC: 11789446. DOI: 10.1002/ijc.35283.

Genome-wide statistical evidence elucidates candidate factors of life expectancy in dogs.

Ko W, Kim S, Catry A, Cho J, Shin S Mol Cells. 2024; 48(1):100162.

PMID: 39580055 PMC: 11721540. DOI: 10.1016/j.mocell.2024.100162.

Spatial characterization and stratification of colorectal adenomas by deep visual proteomics.

Kabatnik S, Post F, Drici L, Bartels A, Strauss M, Zheng X iScience. 2024; 27(9):110620.

PMID: 39252972 PMC: 11381895. DOI: 10.1016/j.isci.2024.110620.

Whole genome sequencing for metastatic mutational burden in extraskeletal myxoid chondrosarcoma.

Zou T, Sethi R, Wang J, Budak G, Chandran U, John I Front Mol Med. 2024; 3:1152550.

PMID: 39086683 PMC: 11285543. DOI: 10.3389/fmmed.2023.1152550.

Small duct and large duct type intrahepatic cholangiocarcinoma reveal distinct patterns of immune signatures.

Bernatz S, Schulze F, Bein J, Bankov K, Mahmoudi S, Grunewald L J Cancer Res Clin Oncol. 2024; 150(7):357.

PMID: 39034327 PMC: 11271402. DOI: 10.1007/s00432-024-05888-y.